Efficacy and determinants of response to HER kinase inhibition in HER2-mutant metastatic breast cancer Journal Article

   


Authors: Smyth, L. M.; Piha-Paul, S. A.; Won, H. H.; Schram, A. M.; Saura, C.; Loi, S.; Lu, J.; Shapiro, G. I.; Juric, D.; Mayer, I. A.; Arteaga, C. L.; de la Fuente, M. I.; Brufksy, A. M.; Spanggaard, I.; Mau-Sørensen, M.; Arnedos, M.; Moreno, V.; Boni, V.; Sohn, J.; Schwartzberg, L. S.; Gonzàlez-Farré, X.; Cervantes, A.; Bidard, F. C.; Gorelick, A. N.; Lanman, R. B.; Nagy, R. J.; Ulaner, G. A.; Chandarlapaty, S.; Jhaveri, K.; Gavrila, E. I.; Zimel, C.; Selcuklu, S. D.; Melcer, M.; Samoila, A.; Cai, Y.; Scaltriti, M.; Mann, G.; Xu, F.; Eli, L. D.; Dujka, M.; Lalani, A. S.; Bryce, R.; Baselga, J.; Taylor, B. S.; Solit, D. B.; Meric-Bernstam, F.; Hyman, D. M.
Article Title: Efficacy and determinants of response to HER kinase inhibition in HER2-mutant metastatic breast cancer
Abstract: HER2 mutations define a subset of metastatic breast cancers with a unique mechanism of oncogenic addiction to HER2 signaling. We explored activity of the irreversible pan-HER kinase inhibitor neratinib, alone or with fulvestrant, in 81 patients with HER2-mutant metastatic breast cancer. Overall response rate was similar with or without estrogen receptor (ER) blockade. By comparison, progression-free survival and duration of response appeared longer in ER+ patients receiving combination therapy, although the study was not designed for direct comparison. Preexistent concurrent activating HER2 or HER3 alterations were associated with poor treatment outcome. Similarly, acquisition of multiple HER2-activating events, as well as gatekeeper alterations, were observed at disease progression in a high proportion of patients deriving clinical benefit from neratinib. Collectively, these data define HER2 mutations as a therapeutic target in breast cancer and suggest that coexistence of additional HER signaling alterations may promote both de novo and acquired resistance to neratinib. SIGNIFICANCE: HER2 mutations define a targetable breast cancer subset, although sensitivity to irreversible HER kinase inhibition appears to be modified by the presence of concurrent activating genomic events in the pathway. These findings have implications for potential future combinatorial approaches and broader therapeutic development for this genomically defined subset of breast cancer.This article is highlighted in the In This Issue feature, p. 161. ©2019 American Association for Cancer Research.
Journal Title: Cancer Discovery
Volume: 10
Issue: 2
ISSN: 2159-8274
Publisher: American Association for Cancer Research  
Date Published: 2020-02-01
Start Page: 198
End Page: 213
Language: English
DOI: 10.1158/2159-8290.Cd-19-0966
PUBMED: 31806627
PROVIDER: scopus
PMCID: PMC7007377
DOI/URL:

https://www.scopus.com/inward/record.uri?eid=2-s2.0-85079077280&doi=10.1158%2f2159-8290.CD-19-0966&partnerID=40&md5=0dd822646eb1113d8c8fc7fe2f4325f9
Notes: Article -- Export Date: 2 March 2020 -- Source: Scopus
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MSK Authors
  1. Gary Ulaner
    147 Ulaner
  2. David Solit
    779 Solit
  3. Sarat Chandarlapaty
    280 Chandarlapaty
  4. David Hyman
    354 Hyman
  5. Komal Lachhman Jhaveri
    202 Jhaveri
  6. Barry Stephen Taylor
    238 Taylor
  7. Alison Michele Schram
    123 Schram
  8. Helen Hyeong-Eun Won
    109 Won
  9. Aliaksandra Samoila
    23 Samoila
  10. Jose T Baselga
    484 Baselga
  11. Maurizio Scaltriti
    170 Scaltriti
  12. Lillian Smyth
    42 Smyth
  13. Sadan Duygu Selcuklu
    29 Selcuklu
  14. Alexander Gorelick
    22 Gorelick
  15. Myra Beth Melcer
    3 Melcer
  16. Yanyan Cai
    16 Cai
  17. Elena Irina Gavrila
    6 Gavrila
  18. Catherine Zimel
    6 Zimel
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